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Erythropoietin molecules to treat acute ischemic stroke: a translational dilemma!

机译:促红细胞生成素分子治疗急性缺血性中风:一个翻译难题!

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IMPORTANCE OF THE FIELD: Since the realization that erythropoietin (EPO) molecules have 'neuroprotective' properties, they have been investigated as treatments for acute ischemic stroke (AIS), but not systematically. The results of the 2009 clinical trial showed that EPO was ineffective as a stroke treatment, and moreover, increased mortality when combined with tissue plasminogen activator. Currently, CEPO, an EPO analog, is entering into a safety, tolerability and pharmacokinetic clinical trial for the treatment of AIS. AREAS COVERED IN THIS REVIEW: This review covers translational and clinical studies carried out over the period 1998 - 2010. WHAT THE READER WILL GAIN: The primary aim of this article is to review the information available regarding the pharmacological and biological characteristics of EPO molecules. Second, based upon the translational research with EPO molecules in preclinical stroke models, a recommendation is made regarding the continued development of EPO molecules as an option to treat AIS. TAKE HOME MESSAGE: EPO, CEPO and helix B peptide EPO analogs have significant neuroprotective activity is preclinical stroke models. However, given the detrimental effect of EPO in a recent clinical trial, preclinical safety studies of EPO molecules in embolic stroke models that parallel acute ischemic stroke in humans are warrented.
机译:领域的重要性:自从认识到促红细胞生成素(EPO)分子具有“神经保护”特性以来,已经对它们进行了研究,以作为治疗急性缺血性中风(AIS)的方法,但尚未系统地进行研究。 2009年临床试验的结果表明,EPO作为中风治疗无效,而且与组织纤溶酶原激活剂联合使用时,死亡率增加。目前,CEPO(一种EPO类似物)正在进入用于AIS治疗的安全性,耐受性和药代动力学临床试验。这篇综述涵盖的领域:这篇综述涵盖了1998年至2010年期间进行的转化和临床研究。读者的收获:本文的主要目的是回顾有关EPO分子的药理和生物学特性的可用信息。其次,基于临床前卒中模型中EPO分子的翻译研究,提出了关于EPO分子作为治疗AIS的选择的持续发展的建议。家庭寄语:EPO,CEPO和螺旋B肽EPO类似物在临床中风模型中具有显着的神经保护活性。然而,鉴于最近一次临床试验中EPO的有害作用,人们迫切希望在与人类急性缺血性中风相似的栓塞性中风模型中进行EPO分子的临床前安全性研究。

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